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Sulfanilamide is mainly used for traumatic infections caused by hemolytic streptococcus and staphylococcus, and local wound infections.
The mechanism of action of sulfanilamide is to interfere with the synthesis of nucleic acids required by pathogenic microorganisms, so that bacteria lack nutrients and stop growing, developing and reproducing. Sulfanilamide have inhibitory effect on hemolytic streptococci, staphylococci and meningococci.
Items | Specification | Result |
| Purity | ≥99.5% | 99.62% |
| Appearance | White crystalline | Conform |
| PH | 5.0-7.0 | 6.0 |
| Heavy metal | ≤20ppm | <20ppm |
| Moisture | ≤0.2% | 0.12% |
| Melting range | 136-140℃ | 136-137℃ |
| Product parameters | |
| Cas number: | 63-74-1 |
| Appearance: | White crystalline |
| Purity: | 99%min |
| Package details: | 25kg/drum |
| Brand: | Fortunachem |
Sulfanilamide is a synthetic antimicrobial drug, recognized as the founding member of the sulfonamide class, commonly known as "sulfa drugs." It marked a revolutionary turning point in medicine, representing one of the first effective, broadly available systemic antibacterial agents, which ushered in the modern antibiotic era.
Sulfanilamide is a bacteriostatic agent, meaning it inhibits bacterial growth rather than directly killing the cells. It acts through competitive inhibition.
Bacteria require para-aminobenzoic acid (PABA) to synthesize folic acid, a vital vitamin for DNA and protein production.
Sulfanilamide, due to its similar chemical structure to PABA, acts as a "false key." It tricks the bacterial enzyme dihydropteroate synthase into using it instead of the real PABA.
This results in the production of a non-functional form of folic acid, halting the bacterial metabolic pathway.
Critically, this mechanism has little effect on human cells because we cannot synthesize folic acid and must obtain it from our diet, making it a selective poison for bacteria.
Sulfanilamide's medical impact in the 1930s was profound. For the first time, doctors had a drug that could effectively treat a wide range of deadly bacterial infections, such as streptococcal septicemia, pneumonia, and meningitis.
However, its history is forever linked to a pivotal tragedy in drug safety. In 1937, the S.E. Massengill Company marketed a liquid preparation of the drug called "Elixir Sulfanilamide." The solvent used was diethylene glycol, a toxic chemical now found in antifreeze. The company's chemists failed to test the safety of this formulation, leading to over 100 deaths from acute kidney failure.
This disaster created massive public outrage and directly catalyzed the passage of the U.S. Federal Food, Drug, and Cosmetic Act of 1938. This landmark legislation, for the first time, required manufacturers to prove the safety of a drug before it could be marketed, fundamentally changing the landscape of pharmaceutical regulation.
While sulfanilamide itself is now largely obsolete in systemic human medicine, having been superseded by more effective and less toxic antibiotics (like penicillin and later generations of sulfa drugs), its derivatives are still used today for various infections. Furthermore, its legacy is immense: it demonstrated the power of systemic antibacterial chemotherapy and its associated tragedy established the essential framework for modern drug safety laws that protect public health globally.
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